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Using acute tryptophan depletion to investigate predictors of treatment response in adolescents with major depressive disorder: study protocol for a randomised controlled trial

机译:使用急性色氨酸耗竭研究重度抑郁症青少年的治疗反应预测因子:一项随机对照试验的研究方案

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Selective serotonin reuptake inhibitors (SSRIs) are amongst the most prescribed antidepressants for adolescents with depressive symptoms and major depressive disorder. However, SSRIs have significant shortcomings as a first-line treatment considering that not all patients respond to these antidepressants. Amongst paediatric populations, meta-analyses indicate that up to approximately 40% of patients do not respond, and for those who do show benefit, there is substantial heterogeneity in response onset. The neurotransmitter serotonin (5-HT) plays a role in the clinical effectiveness and mechanisms of action of SSRIs. However, the exact and complete mechanism of action and reasons for the low response rate to SSRIs in some adolescent populations remains unknown. To examine SSRI response and the role of 5-HT, this study will employ a randomised double-blind within subject, repeated measures design, recruiting adolescent patients with major depressive disorder. Participants will be subjected to acute tryptophan depletion (ATD) and the balanced control condition on two separate study days within a first study phase (Phase A), and the order in which these conditions (ATD/balanced control condition) occur will be random. This phase will be followed by Phase B, where participants will receive open label pharmacological treatment as usual with the SSRI fluoxetine and followed-up over a 12-week period. ATD is a neurodietary method typically used to investigate the impact of lowered brain 5-HT synthesis on mood and behaviour. The major hypothesis of this study is that ATD will be negatively associated with mood and cognitive functioning, therefore reflecting individual serotonergic sensitivity and related depressive symptoms. Additionally, we expect the aforementioned effects of ATD administration on mood to predict clinical improvement with regard to overall depressive symptomatology 12?weeks into SSRI treatment. Australian and New Zealand Clinical Trials Registry (ANZCTR) ACTRN12616001561471 . Registered on 11 November 2016.
机译:选择性5-羟色胺再摄取抑制剂(SSRIs)是患有抑郁症症状和严重抑郁症的青少年处方最广泛的抗抑郁药之一。然而,考虑到并非所有患者对这些抗抑郁药都有反应,SSRIs作为一线治疗存在重大缺陷。在儿科人群中,荟萃分析表明,多达约40%的患者无反应,对于那些表现出获益的患者,反应开始时存在很大的异质性。神经递质血清素(5-HT)在SSRI的临床疗效和作用机制中发挥作用。但是,确切的和完整的作用机理以及某些青少年人群对SSRIs应答率低的原因仍然未知。为了检查SSRI反应和5-HT的作用,本研究将在受试者内部采用随机双盲,重复措施设计,招募患有重度抑郁症的青少年患者。在第一个研究阶段(A期)的两个单独研究日中,参与者将遭受急性色氨酸耗竭(ATD)和平衡控制条件,并且这些条件(ATD /平衡控制条件)的发生顺序将是随机的。此阶段之后是B阶段,参与者将像往常一样接受SSRI氟西汀的开放标签药理治疗,并在12周内进行随访。 ATD是一种神经饮食方法,通常用于研究脑部5-HT合成降低对情绪和行为的影响。这项研究的主要假设是ATD与情绪和认知功能呈负相关,因此反映了个体血清素能敏感性和相关的抑郁症状。此外,我们预期ATD给药对情绪的上述影响可预测SSRI治疗12周后总体抑郁症状的临床改善。澳大利亚和新西兰临床试验注册中心(ANZCTR)ACTRN12616001561471。 2016年11月11日注册。

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